Aldosterone is synthesized in the zona glomerulosa of the adrenal cortex under primary regulation by the renin-angiotensin system. Angiotensin II (A-II) acts through the angiotensin types 1 and 2 receptors (AT1R and AT2R). A-II is metabolized in different tissues by various enzymes to generate two heptapeptides A-III and angiotensin 1-7, which can then be catabolized into smaller peptides. A-II was more potent than A-III in stimulating aldosterone secretion in the adrenocortical cell line HAC15, and A-II, but not A-III, stimulated cortisol secretion. A-II stimulated mRNA expression of steroidogenic acute regulatory protein, 3β-hydroxysteroid dehydrogenase, CYP11B1, and CYP11B2, whereas A-III stimulated 3β-hydroxysteroid dehydrogenase, CYP11B1, and CYP11B2 but decreased the expression of CYP17A1 required for cortisol synthesis. The stimulation of aldosterone secretion by A-II and A-III was blocked by the AT1R receptor blocker, losartan, but not by an AT2R blocker. A-II was rapidly metabolized by the HAC15 cells to mainly to angiotensin 1-7, but not to A-III, and disappeared from the supernatant within 6 h. A-III was metabolized rapidly and disappeared within 1 h. In conclusion, A-II was not converted to A-III in the HAC15 cell and is the more potent stimulator of aldosterone secretion and cortisol of the two. A-III stimulated aldosterone secretion but not cortisol secretion.

译文

:醛固酮是在肾素-血管紧张素系统的主要调控下在肾上腺皮质的肾小球中合成的。血管紧张素II(A-II)通过1型和2型血管紧张素受体(AT1R和AT2R)起作用。 A-II通过各种酶在不同的组织中代谢,生成两种七肽A-III和血管紧张素1-7,然后可以将其分解为较小的肽。在刺激肾上腺皮质细胞系HAC15中的醛固酮分泌方面,A-II比A-III更有效,而A-II(而非A-III)刺激皮质醇分泌。 A-II刺激类固醇生成的急性调节蛋白,3β-羟基类固醇脱氢酶,CYP11B1和CYP11B2的mRNA表达,而A-III刺激3β-羟基类固醇脱氢酶,CYP11B1和CYP11B2但降低了皮质醇合成所需的CYP17A1的表达。 A-II和A-III对醛固酮分泌的刺激被AT1R受体阻滞剂氯沙坦阻断,但未被AT2R阻滞剂阻断。 A-II被HAC15细胞快速代谢,主要代谢为血管紧张素1-7,但不代谢为A-III,并在6小时内从上清液中消失。 A-III快速代谢并在1​​小时内消失。总之,A-II在HAC15细胞中并未转化为A-III,而是对两者的醛固酮分泌和皮质醇更有效的刺激剂。 A-III刺激醛固酮分泌,但不刺激皮质醇分泌。

+1
+2
100研值 100研值 ¥99课程
检索文献一次
下载文献一次

去下载>

成功解锁2个技能,为你点赞

《SCI写作十大必备语法》
解决你的SCI语法难题!

技能熟练度+1

视频课《玩转文献检索》
让你成为检索达人!

恭喜完成新手挑战

手机微信扫一扫,添加好友领取

免费领《Endnote文献管理工具+教程》

微信扫码, 免费领取

手机登录

获取验证码
登录